Decreased CD4 + lymphocytes and innate immune responses in adults with previous extrapulmonary tuberculosis

CD4 + lymphocytes control Mycobacterium tuberculosis infection through cytokine-mediated macrophage activation. Extrapulmonary tuberculosis is presumably a marker of immunodeficiency, but cytokine responses have not been well studied in such patients. Assess immune defects in persons with previous e...

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Bibliographic Details
Published in:Journal of allergy and clinical immunology 2006-04, Vol.117 (4), p.916-923
Main Authors: Antas, Paulo R.Z., Ding, Li, Hackman, Judith, Reeves-Hammock, Linda, Shintani, Ayumi K., Schiffer, Joshua, Holland, Steven M., Sterling, Timothy R.
Format: Article
Language:English
Subjects:
Adult
Biological and medical sciences
CD4 + lymphocytes
CD4 Lymphocyte Count
Cytokines
Cytokines - biosynthesis
extrapulmonary tuberculosis
Female
Fundamental and applied biological sciences. Psychology
Fundamental immunology
HIV
Human immunodeficiency virus
Humans
Immune system
Immunity, Innate
Immunopathology
In Vitro Techniques
Infections
innate immunity
Leukocytes, Mononuclear - immunology
Male
Medical sciences
Middle Aged
Mycobacterium tuberculosis
Tuberculosis
Tuberculosis - immunology
Tuberculosis, Pulmonary - immunology
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Summary:CD4 + lymphocytes control Mycobacterium tuberculosis infection through cytokine-mediated macrophage activation. Extrapulmonary tuberculosis is presumably a marker of immunodeficiency, but cytokine responses have not been well studied in such patients. Assess immune defects in persons with previous extrapulmonary tuberculosis. In vitro cytokine responses of PBMCs from HIV-seronegative adults with previous extrapulmonary tuberculosis (n = 10) were compared with responses from persons with previous pulmonary tuberculosis (n = 24) and latent M tuberculosis infection (n = 30) in a case-control study. Patients and controls did not differ according to age, sex, race, or monocytes. The median time between tuberculosis diagnosis and study entry was 72 and 122 weeks in extrapulmonary and pulmonary patients, respectively ( P = .2). Median CD4 + counts were 660, 814, and 974 lymphocytes/mm 3 in extrapulmonary, pulmonary, and latently infected patients, respectively ( P = .03). At 48 hours, median unstimulated cytokine levels were uniformly lower in extrapulmonary patients than both sets of controls. These differences persisted after controlling for CD4 + count by linear regression analysis. Despite lower unstimulated levels, median TNF-α response was higher in patients with extrapulmonary and pulmonary tuberculosis than latently infected persons after stimulation with PHA 1% ( P = .006) and PHA+IL-12 (1 ng/mL; P = .02); IL-10 remained low in patients with extrapulmonary tuberculosis after the same stimuli ( P = .04 and .06, respectively). There was no primary immunodeficiency in the IL-12/23–IFN-γ axis. HIV-seronegative adults with previous extrapulmonary tuberculosis had lower CD4 + lymphocytes and unstimulated cytokine production. This suggests a subtle abnormality in innate immune function. These characteristics could identify persons at risk for severe tuberculosis manifestations.
ISSN:0091-6749
1097-6825
DOI:10.1016/j.jaci.2006.01.042